Association of functional variations in COMT and GCH1 genes with postherniotomy pain and related impairment

Inna Belfer; Feng Dai; Henrik Kehlet; Peter Finelli; Li Qin; Reinhard Bittner; Eske Kvanner Aasvang

doi:10.1097/01.j.pain.0000460307.48701.b0

Association of functional variations in COMT and GCH1 genes with postherniotomy pain and related impairment

Inna Belfer, Feng Dai, Henrik Kehlet, Peter Finelli, Li Qin, Reinhard Bittner, Eske Kvanner Aasvang

Department of Clinical Medicine

28 Citations (Scopus)

Abstract

Persistent postoperative pain is a well-established clinical problem with potential severe personal and socioeconomic implications. The prevalence of persistent pain varies across surgery types. Severe persistent pain and related impairment occur in 5% to 10% of patients after groin hernia repair. The substantial interindividual variability in pain-related phenotypes within each surgery type cannot be explained by environmental factors alone, suggesting that genetic variation may play a role. We investigated the contribution of COMT and GCH1 to persistent postherniotomy pain (PPP)-related functional impairment. Prospective data from 429 Caucasian male patients with hernia were collected. Three COMT and 2 GCH1 tagging single-nucleotide polymorphisms (SNPs) were genotyped and analyzed for association with PPP-related activity impairment at 6 months after herniotomy. Fifty-five (12.8%) patients had moderate-to-severe pain-related activity impairment 6 months postoperatively as measured by Activity Assessment Scale (≥8.3). Patients with the G allele of COMT SNP rs6269 and C allele of COMT SNP rs4633 had less impairment (P = 0.03 and 0.01, respectively); in addition, the COMT haplotype GCG was associated with less impairment. For GCH1, the A allele of SNP rs3783641, T allele of rs8007267, and AT haplotype showed a protective effect trend (although nonsignificant; P = 0.08, 0.06, and 0.08, respectively). A prediction model of substantial PPP-related activity impairment, combining COMT and GCH1 SNPs with clinical, psychophysical, and psychological risk factors, had a "good" (0.8, area under curve < 0.9) discriminatory power. These data suggest that functional variations in COMT and GCH1 combined with clinical factors are predictive of PPP-related impairment after groin herniotomy.

Original language	English
Journal	Pain
Volume	156
Issue number	2
Pages (from-to)	273-9
Number of pages	7
ISSN	0304-3959
DOIs	https://doi.org/10.1097/01.j.pain.0000460307.48701.b0
Publication status	Published - Feb 2015

Keywords

Adult
Aged
Catechol O-Methyltransferase
GTP Cyclohydrolase
Genetic Association Studies
Genetic Variation
Herniorrhaphy
Humans
Longitudinal Studies
Male
Middle Aged
Pain, Postoperative
Polymorphism, Single Nucleotide
Prospective Studies

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Cite this

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title = "Association of functional variations in COMT and GCH1 genes with postherniotomy pain and related impairment",

abstract = "Persistent postoperative pain is a well-established clinical problem with potential severe personal and socioeconomic implications. The prevalence of persistent pain varies across surgery types. Severe persistent pain and related impairment occur in 5% to 10% of patients after groin hernia repair. The substantial interindividual variability in pain-related phenotypes within each surgery type cannot be explained by environmental factors alone, suggesting that genetic variation may play a role. We investigated the contribution of COMT and GCH1 to persistent postherniotomy pain (PPP)-related functional impairment. Prospective data from 429 Caucasian male patients with hernia were collected. Three COMT and 2 GCH1 tagging single-nucleotide polymorphisms (SNPs) were genotyped and analyzed for association with PPP-related activity impairment at 6 months after herniotomy. Fifty-five (12.8%) patients had moderate-to-severe pain-related activity impairment 6 months postoperatively as measured by Activity Assessment Scale (≥8.3). Patients with the G allele of COMT SNP rs6269 and C allele of COMT SNP rs4633 had less impairment (P = 0.03 and 0.01, respectively); in addition, the COMT haplotype GCG was associated with less impairment. For GCH1, the A allele of SNP rs3783641, T allele of rs8007267, and AT haplotype showed a protective effect trend (although nonsignificant; P = 0.08, 0.06, and 0.08, respectively). A prediction model of substantial PPP-related activity impairment, combining COMT and GCH1 SNPs with clinical, psychophysical, and psychological risk factors, had a {"}good{"} (0.8, area under curve < 0.9) discriminatory power. These data suggest that functional variations in COMT and GCH1 combined with clinical factors are predictive of PPP-related impairment after groin herniotomy.",

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author = "Inna Belfer and Feng Dai and Henrik Kehlet and Peter Finelli and Li Qin and Reinhard Bittner and Aasvang, {Eske Kvanner}",

year = "2015",

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doi = "10.1097/01.j.pain.0000460307.48701.b0",

language = "English",

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journal = "Pain",

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T1 - Association of functional variations in COMT and GCH1 genes with postherniotomy pain and related impairment

AU - Belfer, Inna

AU - Dai, Feng

AU - Kehlet, Henrik

AU - Finelli, Peter

AU - Qin, Li

AU - Bittner, Reinhard

AU - Aasvang, Eske Kvanner

PY - 2015/2

Y1 - 2015/2

N2 - Persistent postoperative pain is a well-established clinical problem with potential severe personal and socioeconomic implications. The prevalence of persistent pain varies across surgery types. Severe persistent pain and related impairment occur in 5% to 10% of patients after groin hernia repair. The substantial interindividual variability in pain-related phenotypes within each surgery type cannot be explained by environmental factors alone, suggesting that genetic variation may play a role. We investigated the contribution of COMT and GCH1 to persistent postherniotomy pain (PPP)-related functional impairment. Prospective data from 429 Caucasian male patients with hernia were collected. Three COMT and 2 GCH1 tagging single-nucleotide polymorphisms (SNPs) were genotyped and analyzed for association with PPP-related activity impairment at 6 months after herniotomy. Fifty-five (12.8%) patients had moderate-to-severe pain-related activity impairment 6 months postoperatively as measured by Activity Assessment Scale (≥8.3). Patients with the G allele of COMT SNP rs6269 and C allele of COMT SNP rs4633 had less impairment (P = 0.03 and 0.01, respectively); in addition, the COMT haplotype GCG was associated with less impairment. For GCH1, the A allele of SNP rs3783641, T allele of rs8007267, and AT haplotype showed a protective effect trend (although nonsignificant; P = 0.08, 0.06, and 0.08, respectively). A prediction model of substantial PPP-related activity impairment, combining COMT and GCH1 SNPs with clinical, psychophysical, and psychological risk factors, had a "good" (0.8, area under curve < 0.9) discriminatory power. These data suggest that functional variations in COMT and GCH1 combined with clinical factors are predictive of PPP-related impairment after groin herniotomy.

AB - Persistent postoperative pain is a well-established clinical problem with potential severe personal and socioeconomic implications. The prevalence of persistent pain varies across surgery types. Severe persistent pain and related impairment occur in 5% to 10% of patients after groin hernia repair. The substantial interindividual variability in pain-related phenotypes within each surgery type cannot be explained by environmental factors alone, suggesting that genetic variation may play a role. We investigated the contribution of COMT and GCH1 to persistent postherniotomy pain (PPP)-related functional impairment. Prospective data from 429 Caucasian male patients with hernia were collected. Three COMT and 2 GCH1 tagging single-nucleotide polymorphisms (SNPs) were genotyped and analyzed for association with PPP-related activity impairment at 6 months after herniotomy. Fifty-five (12.8%) patients had moderate-to-severe pain-related activity impairment 6 months postoperatively as measured by Activity Assessment Scale (≥8.3). Patients with the G allele of COMT SNP rs6269 and C allele of COMT SNP rs4633 had less impairment (P = 0.03 and 0.01, respectively); in addition, the COMT haplotype GCG was associated with less impairment. For GCH1, the A allele of SNP rs3783641, T allele of rs8007267, and AT haplotype showed a protective effect trend (although nonsignificant; P = 0.08, 0.06, and 0.08, respectively). A prediction model of substantial PPP-related activity impairment, combining COMT and GCH1 SNPs with clinical, psychophysical, and psychological risk factors, had a "good" (0.8, area under curve < 0.9) discriminatory power. These data suggest that functional variations in COMT and GCH1 combined with clinical factors are predictive of PPP-related impairment after groin herniotomy.

KW - Adult

KW - Aged

KW - Catechol O-Methyltransferase

KW - GTP Cyclohydrolase

KW - Genetic Association Studies

KW - Genetic Variation

KW - Herniorrhaphy

KW - Humans

KW - Longitudinal Studies

KW - Male

KW - Middle Aged

KW - Pain, Postoperative

KW - Polymorphism, Single Nucleotide

KW - Prospective Studies

U2 - 10.1097/01.j.pain.0000460307.48701.b0

DO - 10.1097/01.j.pain.0000460307.48701.b0

M3 - Journal article

C2 - 25599448

SN - 0304-3959

VL - 156

SP - 273

EP - 279

JO - Pain

JF - Pain

IS - 2

ER -

Association of functional variations in COMT and GCH1 genes with postherniotomy pain and related impairment

Abstract

Keywords

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